Investigation of cystic fibrosis transmembrane conductance regulator variants in South African patients with cystic fibrosis

dc.contributor.advisorPepper, Michael Sean
dc.contributor.coadvisorJoubert, Fourie
dc.contributor.emailu17081786@tuks.co.zaen_US
dc.contributor.postgraduateLe Grange, Odette
dc.date.accessioned2024-01-30T05:34:05Z
dc.date.available2024-01-30T05:34:05Z
dc.date.created2024-04
dc.date.issued2023
dc.descriptionDissertation (MSc (Bioinformatics))--University of Pretoria, 2023.en_US
dc.description.abstractCystic Fibrosis is a genetic disease caused by variants in the CFTR gene. It is one of the most thoroughly studied genetic diseases, with remarkable advances being seen in the ability to diagnose and specifically treat CF patients based on the nature of their variants. Diagnostic protocols have gained in specificity and sensitivity, with high variant detection rates being achieved using new-born screening in populations with higher frequencies of known, common mutations. However, there are several obstacles impeding the improvement of care in LMICs with diverse populations carrying CFTR variants, including challenges in establishing accurate and reliable diagnostics and overcoming misdiagnosis. African populations are known to have high genomic diversity but remain largely understudied. In South Africa, greater knowledge of the CFTR variant spectrum and clinical presentation is needed to enable earlier diagnosis with more specific gene panels, since the variants common to European populations are less frequent in this population. To bridge this gap, next generation sequencing data from a cohort of 60 South African patients and 5 parents of CF patients was used for variant discovery across the exon regions of the CFTR gene. Thereafter, variant effect prediction was performed, and potentially pathogenic variants were identified. Lastly, these potential variants were validated experimentally using Sanger sequencing. Next-generation sequencing of this cohort enabled 27 individuals that were lacking a complete molecular diagnosis to be fully genotyped. 23 confirmed variants have been functionally studied and proven to cause CF; however, 11 variants are yet to have their functional significance characterised. This study demonstrates the extent of diversity that is likely present in the southern African CF population. As the emerging field of precision medicine and the development of specific CFTR therapies gains momentum with the help of high-throughput screening, individuals with CF in LMICs such as South Africa stand to benefit greatly through earlier molecular diagnosis as well as more specific treatment protocols.en_US
dc.description.availabilityUnrestricteden_US
dc.description.degreeMSc (Bioinformatics)en_US
dc.description.departmentBioinformatics and Computational Biology Uniten_US
dc.description.facultyFaculty of Natural and Agricultural Sciencesen_US
dc.description.sponsorshipNRF SAMRC ICMMen_US
dc.identifier.citation*en_US
dc.identifier.doi10.25403/UPresearchdata.25053131en_US
dc.identifier.otherA2024en_US
dc.identifier.urihttp://hdl.handle.net/2263/94153
dc.language.isoenen_US
dc.publisherUniversity of Pretoria
dc.rights© 2023 University of Pretoria. All rights reserved. The copyright in this work vests in the University of Pretoria. No part of this work may be reproduced or transmitted in any form or by any means, without the prior written permission of the University of Pretoria.
dc.subjectUCTDen_US
dc.subjectCystic Fibrosisen_US
dc.subjectNext Generation Sequencingen_US
dc.subjectGenetic diseasesen_US
dc.subjectCFTR genesen_US
dc.subjectSanger sequencingen_US
dc.subjectVariant analysis
dc.subjectGene panel screening
dc.subjectGenetic diversity
dc.subjectGenomics in Africa
dc.subject.otherSustainable Development Goals (SDGs)
dc.subject.otherSDG-03: Good health and well-being
dc.subject.otherNatural and agricultural sciences theses SDG-03
dc.titleInvestigation of cystic fibrosis transmembrane conductance regulator variants in South African patients with cystic fibrosisen_US
dc.typeDissertationen_US

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